Kidins220/ARMS Modulates the Activity of Microtubule-regulating Proteins and Controls Neuronal Polarity and Development

Higuero, Alonso M.; Sánchez‐Ruiloba, Lucía; Doglio, Laura; Portillo, Francisco; Abad‐Rodríguez, José; Dotti, Carlos G.; Iglesias, Teresa

doi:10.1074/jbc.m109.024703

Cited by 57 publications

(56 citation statements)

References 96 publications

(99 reference statements)

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“…Since most hippocampal neurons expressing Kidins220 1-402 did not bear neurites after 1 day in vitro, it is likely that the ankyrin repeats affects neurite initiation, which is important for both dendritic and axonal growth. This is in accordance with previous studies, which showed that Kidins220 regulates dendritic branching in vivo (Wu et al, 2009), and modulated the development of both axons and dendrites (Higuero et al, 2009). In summary, this experiment demonstrates that the inhibitory activity of the ankyrin-rich domain of Kidins220 on neurite outgrowth also occurs in hippocampal neurons, strongly suggesting that the pathway elucidated in PC12 cells has general validity and controls differentiation in primary neurons.…”

Section: The N-terminus Of Kidins220 Inhibits Neurite Outgrowth In Prsupporting

confidence: 82%

Kidins220/ARMS regulates Rac1-dependent neurite outgrowth by direct interaction with the RhoGEF Trio

Neubrand

Thomas

Schmidt

et al. 2010

Journal of Cell Science

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SummaryNeurite extension depends on extracellular signals that lead to changes in gene expression and rearrangement of the actin cytoskeleton. A factor that might orchestrate these signalling pathways with cytoskeletal elements is the integral membrane protein Kidins220/ARMS, a downstream target of neurotrophins. Here, we identified Trio, a RhoGEF for Rac1, RhoG and RhoA, which is involved in neurite outgrowth and axon guidance, as a binding partner of Kidins220. This interaction is direct and occurs between the N-terminus of Trio and the ankyrin repeats of Kidins220. Trio and Kidins220 colocalise at the tips of neurites in NGF-differentiated PC12 cells, where F-actin and Rac1 also accumulate. Expression of the ankyrin repeats of Kidins220 in PC12 cells inhibits NGF-dependent and Trioinduced neurite outgrowth. Similar results are seen in primary hippocampal neurons. Our data indicate that Kidins220 might localise Trio to specific membrane sites and regulate its activity, leading to Rac1 activation and neurite outgrowth.

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Section: The N-terminus Of Kidins220 Inhibits Neurite Outgrowth In Prsupporting

confidence: 82%

Kidins220/ARMS regulates Rac1-dependent neurite outgrowth by direct interaction with the RhoGEF Trio

Neubrand

Thomas

Schmidt

et al. 2010

Journal of Cell Science

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“…PKD1 phosphorylates the scaffold protein Kidins220 [55][56][57][58] . Kidins220 transportation from the TGN to the plasma membrane requires the autophosphorylation of PKD1 at Ser916.…”

Section: Role Of Pkd In Neuronal Polaritymentioning

confidence: 99%

Protein kinase D: a new player among the signaling proteins that regulate functions in the nervous system

Wang

2014

Neurosci. Bull.

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Protein kinase D (PKD) is an evolutionarily-conserved family of protein kinases. It has structural, regulatory, and enzymatic properties quite different from the PKC family. Many stimuli induce PKD signaling, including G-protein-coupled receptor agonists and growth factors. PKD1 is the most studied member of the family. It functions during cell proliferation, differentiation, secretion, cardiac hypertrophy, immune regulation, angiogenesis, and cancer. Previously, we found that PKD1 is also critically involved in pain modulation. Since then, a series of studies performed in our lab and by other groups have shown that PKDs also participate in other processes in the nervous system including neuronal polarity establishment, neuroprotection, and learning. Here, we discuss the connections between PKD structure, enzyme function, and localization, and summarize the recent fi ndings on the roles of PKD-mediated signaling in the nervous system. Keywords: PKD; neuronal polarity; pain modulation; neuroprotection; learning IntroductionMembers of the protein kinase D (PKD) family are diacylglycerol (DAG) and protein kinase C (PKC) effectors.They are activated by the actions of hormones, growth factors, neurotransmitters, and other stimuli through phospholipase C (PLC) [1] . Three widely-expressed mammalian homologs are PKD1 (mouse PKD, human PKCμ) [2,3] , PKD2 [3] , and PKD3 [4] (also named PKC), but the levels of individual PKDs vary in different tissues.Recent fi ndings have revealed that PKDs participate in the regulation of Golgi function through modulating the fi ssion of vesicles from the trans-Golgi network (TGN) [5,6] . Other recent reports have shown that PKDs function during cell proliferation and apoptosis, carcinogenesis, and intracellular trafficking. Here, we describe the connections between PKD structure, enzymatic function, and localization, and then summarize recent fi ndings on the roles of PKD in the nervous system. The PKD Family Belongs to the CaMK GroupThe PKD family comprises PKD1, PKD2, and PKD3. PKD was initially described as an atypical isoform of the PKC family [7] , which is a member of the protein kinase A, G, and C (AGC) serine/threonine kinase subfamily [8,9] . However, later studies revealed that PKD has mixed features of different subclasses of the PKC family, so it does not belong to any one of them. For example, its pleckstrin-homology (PH) domain is closely related to the PKB and G-proteincoupled receptor kinase (GRK) families and is not found in any PKC enzyme, while the cysteine-rich domains are more reminiscent of classical and novel PKCs. The structure and function of the catalytic domain of PKD are quite different from those of the AGC/PKC family members [2][3][4]10] . Indeed, PKD has now been classified as a new family within the (Fig. 1). The elaborate constitution of PKD1 is intricately linked to its catalytic functions, regulation, and intracellular localization (Table 1). PKD1 can be activated through different pathways.First, some stimuli activate PLC, which induces PKD phosp...

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“…Kinase D-interacting substrate of 220 kDa (Kidins220), also known as ankyrin repeat-rich membrane spanning (ARMS), is a protein expressed predominantly in neural tissues. Kidins220 is the fi rst known physiological substrate of protein kinase D (PKD) and has been shown to have a role in determining neuronal polarity (Higuero et al, 2010). Calpain proteolysis infl uences Kidins220 functions and thus may also infl uence neuronal polarity via the PKD pathway (Lopez-Menendez et al, 2009).…”

Section: Role Of Protein Degradation In the Establishment Of Neuronalmentioning

confidence: 99%

Regulation of cell polarity by controlled proteolytic systems

Bórquez¹,

González-Billault²

2011

Biol. Res.

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Epithelial and neuronal cells are highly asymmetric, with discrete regions responsible for different roles that underlie the generation of specifi c compartments within cells that are distinct in biochemical composition, structure, and morphology that ultimately lead to distinct functions. Controlled and specifi c molecular targeting and sorting have been studied to understand the generation of asymmetric domains inside cells. Recently, a new and complementary explanation has emerged to account for the generation of domains that are enriched by a subset of proteins or polarization determinants: local proteolysis. In this review, we discuss the most conspicuous proteolytic systems that may contribute to the generation of cell polarity, namely the ubiquitin-proteosome and the calpain systems. Specifi cally, we focus this review on two cellular processes that depend on the acquisition of cell polarity; cell migration and the establishment of an axon in a neuronal cell.

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Kidins220/ARMS Modulates the Activity of Microtubule-regulating Proteins and Controls Neuronal Polarity and Development

Cited by 57 publications

References 96 publications

Kidins220/ARMS regulates Rac1-dependent neurite outgrowth by direct interaction with the RhoGEF Trio

Kidins220/ARMS regulates Rac1-dependent neurite outgrowth by direct interaction with the RhoGEF Trio

Protein kinase D: a new player among the signaling proteins that regulate functions in the nervous system

Regulation of cell polarity by controlled proteolytic systems

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